Drosophila eIF3f1 mediates host immune defense by targeting dTak1

Author:

Hu Yixuan,Kong Fanrui,Guo HuiminORCID,Hua Yongzhi,Zhu Yangyang,Zhang Chuchu,Qadeer Abdul,Xiao Yihua,Cai QingshuangORCID,Ji ShanmingORCID

Abstract

AbstractEukaryotic translation initiation factors have long been recognized for their critical roles in governing the translation of coding RNAs into peptides/proteins. However, whether they harbor functional activities at the post-translational level remains poorly understood. Here, we demonstrate that eIF3f1 (eukaryotic translation initiation factor 3 subunit f1), which encodes an archetypal deubiquitinase, is essential for the antimicrobial innate immune defense of Drosophila melanogaster. Our in vitro and in vivo evidence indicate that the immunological function of eIF3f1 is dependent on the N-terminal JAMM (JAB1/MPN/Mov34 metalloenzymes) domain. Mechanistically, eIF3f1 physically associates with dTak1 (Drosophila TGF-beta activating kinase 1), a key regulator of the IMD (immune deficiency) signaling pathway, and mediates the turnover of dTak1 by specifically restricting its K48-linked ubiquitination. Collectively, these results provide compelling insight into a noncanonical molecular function of a translation initiation factor that controls the post-translational modification of a target protein.

Funder

MOST | National Natural Science Foundation of China

安徽省科学技术厅 | Natural Science Foundation of Anhui Province

Publisher

Springer Science and Business Media LLC

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